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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Innate immune cells contribute to the IFN-gamma-dependent regulation of antigen-specific CD8+ T cell homeostasis.
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Innate immune cells contribute to the IFN-gamma-dependent regulation of antigen-specific CD8+ T cell homeostasis.

机译:先天性免疫细胞有助于抗原特异性CD8 + T细胞稳态的IFN-γ依赖性调节。

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摘要

IFN-gamma has a dual function in the regulation of T cell homeostasis. It promotes the expansion of effector T cells and simultaneously programs their contraction. The cellular mechanisms leading to this functional dichotomy of IFN-gamma have not been identified to date. In this study we show: 1) that expansion of wild-type CD8+ T cells is defective in IFN-gamma-deficient mice but increased in IFN-gammaR-deficient mice; and 2) that contraction of the effector CD8+ T cell pool is impaired in both mouse strains. Furthermore, we show that CD11b+ cells responding to IFN-gamma are sufficient to limit CD8+ T cell expansion and promote contraction. The data presented here reveal that IFN-gamma directly promotes CD8+ T cell expansion and simultaneously induces suppressive functions in CD11b+ cells that counter-regulate CD8+ T cell expansion, promote contraction, and limit memory formation. Thus, innate immune cells contribute to the IFN-gamma-dependent regulation of Ag-specific CD8+ T cell homeostasis.
机译:IFN-γ在调节T细胞稳态中具有双重功能。它促进效应T细胞的扩增并同时编程其收缩。迄今为止尚未发现导致这种功能性二分法干扰素-γ的细胞机制。在这项研究中,我们显示:1)野生型CD8 + T细胞的扩增在IFN-γ缺陷小鼠中是有缺陷的,但在IFN-γR缺陷小鼠中却增加了; 2)在两种小鼠品系中,效应CD8 + T细胞库的收缩均受到损害。此外,我们显示响应IFN-γ的CD11b +细胞足以限制CD8 + T细胞扩增并促进收缩。此处提供的数据表明,IFN-γ可直接促进CD8 + T细胞的扩增,并同时诱导CD11b +细胞中的抑制功能,这些功能可反调节CD8 + T细胞的扩增,促进收缩并限制记忆形成。因此,先天性免疫细胞有助于Ag特异性CD8 + T细胞稳态的IFN-γ依赖性调节。

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